One of the things that civil liberties activists like to lament about is that the general public seems to care more about Google and Facebook using their personal data to target advertising than the government using it to target drone strikes.

The reality is that both types of abuse are dangerous, and they work hand in hand.

It's hard to find a more perfect example of this collusion than in a bill that's headed for a vote soon in the U.S. Senate: the Cybersecurity Information Sharing Act, or CISA.

CISA is an out and out surveillance bill masquerading as a cybersecurity bill. It won't stop hackers. Instead, it essentially legalizes all forms of government and corporate spying.

Here's how it works. Companies would be given new authority to monitor their users -- on their own systems as well as those of any other entity -- and then, in order to get immunity from virtually all existing surveillance laws, they would be encouraged to share vaguely defined "cyber threat indicators" with the government. This could be anything from email content, to passwords, IP addresses, or personal information associated with an account. The language of the bill is written to encourage companies to share liberally and include as many personal details as possible.

That information could then be used to further exploit a loophole in surveillance laws that gives the government legal authority for their holy grail -- "upstream" collection of domestic data directly from the cables and switches that make up the Internet.

Thanks to Edwards Snowden, we know that the NSA, FBI, and CIA have already been conducting this type of upstream surveillance on suspected hackers. CISA would give the government tons of new domestic cyber threat indicators to use for their upstream collection of information that passes over the Internet. This means they will be gathering not just data on the alleged threat, but also all of the sensitive data that may have been hacked as part of the threat. So if someone hacks all of Gmail, the hacker doesn't just get those emails, so does the U.S. government.

The information they gather, including all the hacked data and any incidental information that happens to get swept up in the process, would be added to massive databases on people in the U.S. and all over the world that the FBI, CIA, and NSA are free to query at their leisure. This is how CISA would create a huge expansion of the "backdoor" search capabilities that the government uses to skirt the 4th Amendment and spy on Internet users without warrants and with virtually no oversight.

All of this information can be passed around the government and handed down to local law enforcement to be used in investigations that have nothing to do with cyber crime, without requiring them to ever pull a warrant. So CISA would give law enforcement a ton of new data with which to prosecute you for virtually any crime while simultaneously protecting the corporations that share the data from prosecution for any crimes possibly related to it.

There's little hope for ever challenging this system in court because you'll never know if your private information has been shared under CISA or hoovered up under a related upstream collection. In a particularly stunning display of shadyness, the bill specifically exempts all of this information from disclosure under the Freedom of Information Act or any state, local, or tribal law.

The members of Congress who are pushing hardest for the bill, unsurprisingly, have taken more than twice as much money from the defense industry than those who are opposing it. These politicians claim that CISA is intended to beef up U.S. cybersecurity and stop foreign hackers from ruining everything, but, as their funders in the defense industry know well, it will really just give the government more data and create new opportunities for contractors to sell their data analysis services.

The world's cybersecurity experts say that CISA won't stop cyber attacks, but it will create a gaping loophole for law enforcement agencies from the NSA right down to your local police department to access people's private information without a warrant. Systems like this have chilling effects on our willingness to be ourselves and speak openly on the Internet, which threatens our most basic rights.

The Internet makes a lot of good things possible, but it also makes it possible for corporations and governments to exploit us in ways they never could before. The debate over CISA is not about hackers, or China, or cybersecurity -- it's about whether we want to further normalize ubiquitous monitoring, warrantless surveillance, and unfettered manipulation of our vulnerabilities, or if we want to protect the Internet as a promising platform for freedom and self expression.

Last week a Russian White Dragon Society representative came to Japan to cement an alliance with other factions of the WDS around the world. As a part of this, the WDS authorized the release of this photograph:
The person pictured with this writer (in his capacity as WDS spokesperson) is Masaaki Hatsumi. Hatsumi runs the Bujinkan martial arts training school, which has trained over 250,000 special operations troops and has a network of 50 training centers worldwide. His name is a household word among people involved in actual fighting and real martial arts worldwide. He trains FBI, British, US, Russian, Iranian and other Special Forces. Chinese sources say he is the only Japanese citizen who has free access to the top levels of the Chinese government. At the meeting, Hatsumi expressed support for WDS goals.

The alliance of the world’s top fighting forces has spelled doom for the Khazarian mafia and their rapidly shrinking coterie of slave politicians. In particular, the Pentagon has begun coordinating with the Russians against the Khazarian mafia and multiple politicians who have been bribed by the Khazarian mob.

Last week again, multiple developments around the world made it very clear the worldwide Khazarian mafia control grid continues to be dismantled. For example, the Pentagon issued a photograph of Defense Secretary Ashton Carter with top Khazarian mobster and war criminal Benyamin Netanyahu showing a clearly distraught and angry Netanyahu.

As we wrote last week, he was read the riot act. He was told Israel’s “Iron Dome” anti-missile defenses had been rendered useless and Israel was defenseless. Netanyahu was forced to
hand over 16 Cobra helicopters to Jordan and pay big money to buy accident prone Ospreys from the Americans.

After Carter left, Israel’s military and intelligence establishment made public moves to distance themselves from the criminal Netanyahu.

The Carter visit was followed by a heavy duty assault against Israel’s proxy ISIS forces in the Middle East. The Saudis arrested 431 Khazarian ISIS agents while the Turks arrested 251. This was followed by US bombers flying out of Turkey to attack ISIS forces in Syria while avoiding attacks on Syrian government troops.

In the Ukraine, meanwhile, the Russians have accumulated over 2500 pages of war crimes evidence against the Khazarian Nazi Ukrainian regime. The Pentagon is helping dismantle the Nazi network in the Ukraine in exchange for Russian help in the Middle East and Iran. That is why there were reports of military attacks against the Nazi army in the Ukraine last week. Needless to say, States Department Nazi Victoria Nuland and here Khazarian bosses are in deep trouble and will be headed for jail as a result of their criminal actions in the Ukraine.

There were also new moves against the Khazarian mafia in the United States. The ongoing efforts to force Hitlery Clinton to face criminal charges of “using a private computer for secret government work” are just a cover for more serious charges like mass murder. The outing of John McCain as a traitor and not a war hero is another part of this campaign against Khazarian mafia henchmen in Washington DC.

The recent Congressional move to take citizenship away from Americans who support terrorism was passed at Pentagon request and is aimed mainly at Israeli/US double citizens engaged in troublemaking, a Pentagon source says.

Also, increasing pressure is being put on house slave acting president Barack Obama to not only release hidden information about 911 and 311 but also to release information about Malaysian air flight 17. Release of information about the shooting down of flight 17 will implicate Israel, Jeb Bush and Obama himself, multiple agency sources concur.

The revelations about the eugenics and population control Bush/Rockefeller front, Planned Parenthood, selling organs of aborted fetuses was another aspect of the attack against the Khazarian Satanic network. There will be more revelations about missing children and other evil acts in the US coming out as multiple investigations close in on all sides against the Khazarians, according to Vatican P2 sources.

Moves to dismantle Khazarian mafia control of the major media companies are also underway. The Rothschild’s sold off their stake in the Financial Times Newspaper to the Japanese Nikkei group as a way of cashing out before having their media control confiscated by anti-trust action, according to MI5 sources. The Nikkei group is employee owned and promise the FT will have editorial independence. Having worked for the Nikkei in the past, I can say they are editorially timid and not very international minded but, they will probably keep their word about FT editorial independence.

Another move against Khazarian media control was the blocking of efforts by the Comcast Corporation to take over Time Warner Cable. Time Warner will be taken over by a group not affiliated with the Khazarian mafia. The EU has further acted by filing an anti-trust action against 6 major Hollywood studios. The Chinese have also moved in on Hollywood and have already made major changes to the content of the movies produced there.

The moves against Khazarian control of the media will continue to intensify over the coming months, multiple sources said. The Rothschilds are also, for example, now trying to find a buyer for their flagship magazine “the Economist” also known as “the Imperialist.” Chinese and Japanese buyers are sniffing around. The other Khazarian press barons too, will soon be under strong pressure to either start publishing the unvarnished truth or get out of the media business, according to WDS sources.

Some of the British press is already waking up to the new reality and have begun to release hitherto taboo information. For example, Lord Sewel was forced to resign from the House of Lords after photographs of him snorting cocaine with prostitutes appeared in the press.

Lord Sewel is a key ally of former British Prime Minister Tony Blair. His resignation will help pave the ground for more resignations and arrests culminating in pedophile and murder charges being made against former Prime Minister Tony Blair, according to MI5 agents. Tony Blair, of course, is one of the top Bush/Nazi faction agents in the UK so his arrest will lead to other, higher ranked criminals.

The move against Sewel was followed by erroneous reports on US internet news sites about the death of Queen Elizabeth. Photographs of the Queen making a Nazi salute as a young child were also released in the corporate press. The Queen is fine, has been photographed in public recently and is not about to be intimidated, according to MI5. Nonetheless, the Queen would be well advised to release all information about her family’s links with the Nazis and Hitler before it is released by other, not necessarily friendly, sources.

The various political and military moves against the Khazarians coincided with intensified economic and financial warfare. Citibank and JP Morgan have been pushing down worldwide commodities prices with heavy selling in the futures markets. The result has been a huge slump in commodities prices, notably oil, silver, copper and gold. This slump has continued even though physical demand remains strong. The fact that there was illegal manipulation of the gold futures market aimed at pushing the price of gold down shows how desperate the cabalists are to push its price down.

This appears to be aimed against China because Chinese have been accumulating as many physical assets as they can as part of their move to take control of the financial system away from the Khazarian mob. The Chinese have responded to this commodities move by dumping over $520 billion in US treasuries in the past 5 quarters according to JP Morgan.

The WDS believes that neither the Chinese communist government nor the Khazarian mafia should be in charge of the world’s financial system. Instead, all the criminal parts of the private banking system need to be shut down and nationalized. There also needs to be a return to the historical norm of government controlled currency, not Khazarian (or Chinese) gangster control.

Military types like to have a clear target when they take action. The answer is they need to take over the Federal Reserve Board, the European Central Bank and the Bank of Japan. This would only require about 1000 special forces troops, at the most, to accomplish.

Taking over these institutions can be done in a way that does not disrupt the real economy. Furthermore, confiscating assets illegally taken from the people by Khazarian gangsters will lead to an unprecedented boom. In Japan alone, the amount of money stolen by Khazarian gangsters over the past decade would be worth $100,000 for every man, woman and child in the country. In the US the sum stolen by gangsters pretending to be central bankers would be even greater. In criminal law it is a given that stolen assets need to be returned to their rightful owners. These owners are the average tax-paying citizens of the planet. Police and military agencies around the world have a duty to enforce the law and arrest criminals. Top central bankers are proven criminals. So, what are we waiting for?

Anonymous “now privy to many of Stephen Harper’s most cherished secrets”

“We will still maintain access to information highly damaging to Stephen Harper and other supporters of Bill-C51″

Hacktivist group Anonymous has started releasing high-level documents retrieved from secure Harper government computers as retaliation for the RCMP’s recent murder of one of its members.

On Monday, the group released a document it claimed to have retrieved from the Treasury Board of Canada. The document, dated Feb, 2014, details the Harper government plans to boost the domestic and foreign capabilities of the Canadian Security Intelligence Service (CSIS) and other key spy agencies.

“We repeat our insistence upon the immediate arrest of the RCMP killers of James McIntyre,” Anonymous said in a press release and the video above, both released Monday. “Unless and until that happens, we will be releasing stunning secrets at irregular intervals.”

But the international hacktivist group’s concerns stretch far beyond the call for justice for McIntyre, an Anonymous activist who was gunned down by the RCMP in Dawson Creek, British Columbia, earlier this month.

“Stephen Harper, Canadian security forces, and their corporate overlords have now determined that anyone opposing their fossil fuel agenda is a terrorist,” Anonymous said in its press press release and video. “Canada has made opposing fossil fuel mania with action, words or thoughts into a summary criminal offense of the highest order.”

The group is also irked by Harper’s new anti-terror legislatio, Bill C-51, which will transforms CSIS into a dictatorship-style secret police force operating with neither oversight nor accountability. Rights groups have argued that C-51 will grant Canada’s spy and policing agencies the power to violate the Canadian Charter of Rights and Freedoms. Last month, Anonymous downed several Canadian government websites as part of a protest against C-51.

Until now, the government has publicly acknowledged the existence of three foreign CSIS spy stations, based in London, Paris and Washington. Anonymous puts the number at 25.

Then the most stunning part of the hacktivist group’s disclosures: Harper ordered the secretive Communications Security Establishment (CSE) to spy on U.S. President Barack Obama. The Americans uncovered the operation and retaliated by thwarting the Keystone XL tar sands pipeline, the group claims.

Canada has made opposing fossil fuel mania with action, words or thoughts into a summary criminal offense of the highest order.

Anonymous has been collecting bits of evidence and making plans for many months. Beginning in June, we launched an all out assault on Canada’s Internet infrastructure in opposition to C-51, Canada’s secret police bill.

We are also concerned that Stephen Harper and the Conservative Party of Canada will once again use widespread cheating in the upcoming federal elections.

Meanwhile, Canadian security forces and their Five Eyes partners in New Zealand, the UK, Australia, and the U.S. have been extremely pro-active in developing and purchasing offensive hacking capabilities.

Fortunately for us, Canada has been far more lax in defending its own systems. We have just released a secret document from the Canadian cabinet. We are excluding certain document security features, and, accordingly, some heading material. This is a painstaking process. We simply cannot release a document for every story we will be reporting over the coming months.

This first document, though, combined with remarks from Tony Clement after our DDoS attacks last month, show that Harper’s cabinet made direct decisions domestically, as well as for foreign spy stations, to update security systems at a leisurely pace over at least a four year period.

Congratulations! You left many doors open for us!

We are now privy to many of Stephen Harper’s most cherished secrets.

For instance, shortly after winning a majority in 2011, the NSA discovered that Stephen Harper had grown a bit to big for his Christian britches. He and the Canadian Security Establishment were attempting to spy on their Five Eyes partners in the U.S. Obama’s top intelligence officials were furious when they caught CSE in the act. They vowed to kill off Harper’s number one priority, the KXL pipeline.

By the way, Mr. Stephen Blaney, there is nothing more undemocratic than repeatedly cheating at elections then cutting the budget for the elections watchdog. All the while, your government has continued with unprecedented secrecy, antipathy to legitimate media inquiry, and outright contempt independent scientific inquiry.

We repeat our insistence upon the immediate arrest of the RCMP killers of James McIntyre. Unless and until that happens, we will be releasing stunning secrets at irregular intervals. Of course, even if such arrests take place, we will still maintain access to information highly damaging to Stephen Harper and other supporters of Bill-C51.

Enjoy the summer, everyone. Fall will be Wild.

Until then:We Are Anonymous. Expect Us. All your secrets are belong to the mask.

A controversial design for a new, advanced type of space travel received a boost as German scientists confirmed that it does in fact work.

The EMDrive propulsion system would permit travel at speeds until now only seen in science fiction.

When the concept was first proposed it was considered impossible because it went against the laws of physics.

But subsequent tests - further backed up by this announcement - have shown that the idea could revolutionise space travel.

Martin Tajmar, professor and chair for Space Systems at the Dresden University of Technology confirmed that the EMDrive would work. Pictured is the first device created by Roger Sawyer

Researchers say the new drive could carry passengers and their equipment to the moon in as little as four hours.

A trip to Alpha Centauri, which would take tens of thousands of years to reach right now, could be reached in just 100 years.

The system is based on electromagnetic drive, or EMDrive, which converts electrical energy into thrust without the need for rocket fuel.

Martin Tajmar, professor and chair for Space Systems at the Dresden University of Technology, presented his work at the American Institute for Aeronautics and Astronautics' Propulsion and Energy Forum in Orlando yesterday.

The website Hacked obtained a copy of Tajmar's Propulsion and Energy Forum paper.

'Our measurements reveal thrusts as expected from previous claims after carefully studying thermal and electromagnetic interferences,' wrote Tajmar in the paper, according to the website.

'If true, this could certainly revolutionise space travel.'

NASA'S BIGGEST EVER ROCKET

The Space Launch System (SLS) is set to usher in a new era of exploration to destinations beyond Earth's orbit.

When it's built in 2018, it will launch astronauts in the agency's Orion spacecraft on missions to an asteroid placed in lunar orbit, and eventually to Mars.

Now, engineers are one step closer to that goal after last week completing a major design review for what will eventually be the world's biggest and most powerful rocket.

The in-depth review – the first in almost 40 years for a Nasa exploration class vehicle - provides a final look at the design of the rocket before full-scale construction begins.

While there has been some scepticism surrounding the EMDrive, in April Nasa released results of their own test which showed that the EMDrive did in fact create thrust.

'Thrust measurements of the EMDrive defy classical physics’ expectations that such a closed (microwave) cavity should be unusable for space propulsion because of the law of conservation of momentum,' announced NasaSpaceFlight.com in April

The site has become an unofficial source of EMDrive news, with Nasa engineers reportedly posting on its forum.

The announcement will add momentum to developing a working EMDrive, as Tajmar is considered an ideal candidate to test the controversial system due to his 'well-equipped lab and a strong background in tracking experimental error,' according to Wired.

Tajmar wrote: 'Additional tests need to be carried out to study the magnetic interaction of the power feeding lines used for the liquid metal contacts.'

'Nevertheless, we do observe thrusts close to the magnitude of the actual predictions after eliminating many possible error sources that should warrant further investigation into the phenomena.

According to classical physics, the EMDrive should be impossible because it seems to violate the law of conservation of momentum.

The law states that the momentum of a system is constant if there are no external forces acting on the system – which is why propellant is required in traditional rockets.

'Our measurements reveal thrusts as expected from previous claims after carefully studying thermal and electromagnetic interferences,' wrote Tajmar in the paper. Pictured is an illustration from the paper

Researchers from the US, UK and China have demonstrated EMDrives over the past few decades, but their results have been controversial as no one has been exactly sure how it works.

But earlier this year, Nasa built an EMDrive that works in conditions like those in space, according to users on forum NasaSpaceFlight.com.

A number of those discussing the plan on the technical forum claim to be Nasa engineers who are involved in the project.

While there has been some scepticism around the EMDrive, in April Nasa released results of their own test which showed that the EMDrive did in fact create thrust. Martin Tajmar has said the findings could revolutionise space travel. Pictured is his experimental set-up to test the system

The concept of an EmDrive engine is relatively simple. It provides thrust to a spacecraft by bouncing microwaves around in a closed container.

Solar energy provides the electricity to power the microwaves, which means that no propellant is needed.

The implications for this could be huge. For instance, current satellites could be half the size they are today without the need to carry fuel.

Humans could also travel further into space, generating their own propulsion on the way.

When London-based Roger Sawyer came up with concept in 2000, the only team that took him seriously was a group of Chinese scientists.

In 2009, the team allegedly produced 720 millinewton (or 72g) of thrust, enough to build a satellite thruster. But still, nobody believed they had achieved this.

Researchers in Osaka were able to produce a 2-petawatt laser beam using a device known as the Laser for Fast Ignition Experiment (LFEX).

The power of the 'Death Star'-like beam is equivalent to 1,000 times the world's total electricity consumption, the scientists claim.

The 328ft (100 metre)-long LFEX device has strategically-placed glass panels that are used to amplify the laser beam. The team were able to produce such a high output by concentrating the power to 1 pico-second, or around a trillionth of a second

While it produced a huge amount of power, the energy required for the beam itself is equivalent to that needed to power a microwave for two seconds.

The team were able to produce such a high output from low energy by only firing the laser beam for 1 pico-second, or a trillionth of a second.

To amplify the beam's power, energy was applied to strategically-placed glass panels along the 328ft (100 metre)-long LFEX device.

These glass lamps were able focus the beam to boost its energy as it passed through.

In the experiment, energy was applied to glass sections using devices similar to fluorescent lamps. These glass lamps were used to boost the energy of the beam as it passed through

HOW POWERFUL IS IT?

The device produced a 2-petawatt - or 2 quadrillion-watt - laser beam.

This is equivalent to 1,000 times the world's electricity consumption.

To put that in context, Rheinmetall Defense was recently able to shoot a drone down a mile away using a 50kW laser.

The 50kW laser was 10 billion times less powerful that the one used in Japan.

Up until today's announcement, the world has only ever within a 1-pettawatt laser created by the University of Texas, Austin.

'With heated competition in the world to improve the performance of lasers, our goal now is to increase our output to 10 petawatts,' said the institute's Junji Kawanaka, an associate professor of electrical engineering at the university

To put that into context, according to Popular Science, a 50,000 watt laser successfully took down a drone just a mile away.

That 50kW laser was 10 billion times less powerful that the one used in Japan.

Up until today's announcement, the world has only ever witnessed a 1-pettawatt laser created by the University of Texas, Austin.

Not only did the Japanese laser generate twice as much power, but the team says it also has 100 times as much energy as its Texas rival.

The laser, liked to the Death Star laser in Star Wars, is currently mainly of scientific interest rather than having any real-world purpose.

Researchers in Osaka were able to produce a 2-petawatt - or 2 quadrillion-watt - laser beam using the Laser for Fast Ignition Experiments (LFEX). This is equivalent to 1,000 times the world's electricity consumption, causing the laser to be compared to that on the Death Star in Star Wars (pictured

INVESTIGATION: Three days before Dr. Bradstreet was found dead in a river, U.S. govt. agents raided his research facility to seize a breakthrough cancer treatment called GcMAF

(NaturalNews) The history of the suppression of medical science in America is a long one, filled with true accounts of pioneering doctors and clinicians being threatened, intimidated and even assassinated in order to bury emerging cures and keep the "sick care" industry in control. (The American Medical Association, for example, has been found guilty by the U.S. federal courts of a conspiracy to destroy the chiropractic industry, by the way.)

Over the last few days, we've learned that before being found shot in the chest and floating in the river, pioneering medical researcher Dr. Bradstreet was working with a little-known molecule that occurs naturally in the human body. Called, "GcMAF", this molecule has the potential to be a universal cancer cure for many people. It has also been shown to reverse signs of autism in the vast majority of patients receiving the treatment.

While GcMAF is perfectly legal as a treatment in dozens of advanced nations around the world, the U.S. Food and Drug Administration has outlawed it, calling it an "unapproved drug." It is with this designation -- an effort to suppress the forward progress of medical science -- that the U.S. government conducted a raid on Dr. Bradstreet's clinic, specifically seeking to confiscate GcMAF in order to shut down his research and halt his treatment of patients. Meanwhile, Big Pharma gets special permission to unleash untested, experimental drugs on the public as long as those drugs earn sufficient profits.

In this article, I summarize the videos, articles and documents covering GcMAF and the mysterious death of Dr. Bradstreet. An exhaustive investigation needs to be pursued on this matter, possibly involving private investigators. The timing and manner of Dr. Bradstreet's death seems highly suspicious, especially in light of the many other holistic doctors who have recently been found dead under mysterious circumstances. (Dr. Nicholas Gonzalez died just days ago...)

Is there a motive for the murder of pioneering cancer researchers working on a possible universal cancer cure? Of course there is... it's the most common motive in the world: MONEY.

A universal cancer cure would destroy the profitability of the highly lucrative cancer industry and collapse the American Cancer Society, hospitals, oncology clinics and pharmaceutical companies that depend on chemotherapy revenues to stay profitable. Key to their profitability is the inescapable fact that conventional cancer treatments simply don't work most of the time, creating a reliable profit stream of repeat business from patients who are never cured (by design).

EzekielDiet.com story that covers the apparent series of murders of holistic doctors, many of whom are working on advanced treatment protocols that render high-profit sectors of conventional medicine OBSOLETE:

Yet another doctor was just found murdered inside his home here on the East Coast of Florida. This makes six doctors to be found dead in the last month just from this region of the country alone. Four out of the six were found dead here in Florida. We lost the holistic Dr. Teresa Sievers, MD, who was found murdered in her Florida home just weeks ago. We've also lost the alternative Dr. Jeff Bradstreet, MD, who was found in a river with a gunshot to his chest. He'd recently moved to Georgia from Florida. We've also lost the Osteopath. Dr. Riley, who was found in Georgia at her home; just a few hours from the Florida border. She was found with a gunshot wound to her head.

Now we've lost Dr. Schwartz MD, who was found murdered in his home, on Sunday, July 19th, 2015. This was four weeks to the day after the death of the first physician: (Dr. Bradstreet MD) who I broke the story on a month ago. His family is still seeking answers as to what happened to him and they're some of the kindest people I know. The latest MD, Dr. Schwartz, in the picture above, lived just north of the fit, healthy, holistic Dr. Hedendal; who was the second doctor to be found dead this past Father's Day, in Boca Raton. This was the same day that Dr. Holt died at the age of 33. Both were fathers; and again, both men died here in Florida on June 21st, 2015.

After about 16-22 administrations (approximately 3.5-5 months) of GcMAF, these patients had insignificantly low serum enzyme levels equivalent to healthy control enzyme levels, ranging from 0.38 to 0.63 nmole/min/mg protein, indicating eradication of the tumors. This therapeutic procedure resulted in no recurrence for more than 4 years.

In other words, the administration of GcMAF eradicated tumors and left patients cancer-free for 4+ years with no additional treatment!

Both U.S. and UK governments desperately seizing all supply, shutting down clinics, even as millions die from cancer every decade...

More than 10,000 vials were seized at this site and production of this unlicensed medicine has now ceased. These products were sold through various European websites and UK patients may have bought it from one of these websites. We are working with colleagues in other countries to alert them to the potential risks. Our investigations are ongoing and we have received no reports to date of side effects caused by this product.

That same page lists some of the websites where GcMAF had been available for purchase:

GcMAF (Gc Protein derived Macrophage Activating Factor) - Gc MAF treatment is a highly effective macrophage activating therapy, used to stimulate the immune system and activate macrophages so that they can destroy cancer cells and other abnormal cells in the body.

What exactly is Second Generation GcMAF?High Dose Second Generation Gc-MAF is produced using our new Patent Pending process which was developed here in Japan by Saisei Mirai in collaboration with Dr Hitoshi Hori and Dr Yoshihiro Uto at the University of Tokushima who have been studying GcMAF for over 20 years. Studies on GcMAF began at the University of Tokushima in 1992, after they were introduced to Dr Nobuto Yamamoto's work and a collaboration began...

Second Generation GcMAF is made using a new and improved 2nd generation method of Gc-MAF production which is 10-20 times more concentrated and is more active and stable than other GcMAF that is currently available. Importantly, this much higher concentration GcMAF has been clinically demonstrated to be largely free of any side effects in the great majority of patients and is much more stable because it is resistant to oxidation.

That same site describes Oral GcMAF as follows: "Oral GcMAF is a form of GcMAF produced from bovine colostrum by Saisei Mirai which was developed in collaboration with Tokushima University."

It also lists the following health conditions as being treatable with GcMAF, potentially a "universal cancer cure" substance:

Gc-MAF and/or oral Colostrum MAF macrophage activation therapy is indicated in the treatment of any diseases where there is immune dysfunction or where the immune system is compromised, such as:

Do you see yet why the medical establishment must SUPPRESS GcMAF and destroy all knowledge of its clinical applications? This one substance holds the potential to render numerous vaccines and pharmaceuticals utterly obsolete.

A clinical study out of Italy on 94 children with autism showed that 83 of them made considerable progress while on GcMAF. The most common reported improvements involve:

• Cognitive abilities including attention and focus, learning and understanding, receptiveness and awareness of the environment and both receptive and expressive language gains.

• Social Skills including willingness to interact and communicate with peers.

• Behavior including less hyperactivity, less stereotypical behaviors and improved cooperation and compliance.

In another study of 1500 children with autism, 85% had high levels of viruses and a compromised immune system. All 1500 received weekly GcMAF injections and 70% of the children responded to the treatment with reduced symptoms and another 15% made full recoveries. The other 15% did not respond.

It was stated that the reduction of autistic symptoms is permanent provided that GcMAF has been taken long enough for the body to produce its own GcMAF which typically takes 24 weeks.

Back in 1993, Nobuto Yamamoto, then working at Temple University School of Medicine in Philadelphia, PA, USA, first described a remarkable molecule. His paper reported the conversion of vitamin D3 binding protein (DBP, known in humans as Gc) into a potent macrophage-activating factor (MAF), known as Gc-MAF. Macrophages are a key part of the human immune system with two roles: to engulf and destroy pathogens and cellular debris, and to recruit other immune cells to respond to the pathogen.

Gc-MAF hasn't had the benefit of a single patent owner – as a natural molecule, it cannot be patented without being modified – with the will and resources to push it under the noses of the public and health authorities. Dr Yamamoto has run small human trials in breast, prostate and colorectal cancers, with promising results.

David Noakes might just be the person to bring Gc-MAF into the mainstream. He's the CEO of Immuno Biotech Ltd. and spokesperson for First Immune Gc-MAF, a project he describes as, "PhD and BSc biochemists and biomedical scientists... with external doctors, oncologists and scientists who kindly provide advice, committed to bringing some of the increasing number of published but relatively unused medical cures to as many people as we can." At the moment, Noakes and his colleagues are supplying Gc-MAF to 30 countries where it is legal, via a network of "around 300" doctors. Their Gc-MAF is made to extremely high standards, and is being used in ongoing clinical research by Noakes' collaborators and others. Their ultimate goal is to, "Build the case that GcMAF is effective for various illnesses, which will help to make it available to the public".

GcMAF suppliers fighting for survival against a global medical monopoly that profits from disease

The medical laws have been changed over the last 40 years so that all the brilliant breakthroughs in cancer are denied to the British public. Lord Maurice Saatchi had to watch his wife die, while his doctor told him the only thing he was allowed to prescribe her was chemotherapy, which would shorten her life. He hopes to bring the Medical Innovation Bill to Parliament, so instead of obeying a destructive government law, a doctor will be able to prescribe whatever treatment is best for the patient...

Bad law kills, and Britain has the worst medical laws in Europe. The 1939 Cancer Act makes it illegal to discuss the possibility cancer can be cured, which is partly why 160,000 people die unnecessarily of cancer in Britain every year. Science and treatments are decades ahead of where the medical industry is today. The MHRA's job is to get life saving treatments like GcMAF out to people as quickly as possible. Instead they block them to protect billion dollar Big Pharma monopolies, who also fund the MHRA. Over a hundred thousand lives could be saved every year if the 1939 Cancer Act were repealed, and the MHRA were closed down.

There are 142 eminent scientists who have published GcMAF research papers on the US National Library of Medicine alone.

Your GcMAF empowers your body to cure itself. In a healthy person your own GcMAF has 11 actions discovered so far, including two on cells, three excellent effects on the brain, and 6 on cancer. Amongst these it acts as a "director" of your immune system. But viruses and malignant cells like cancer send out an enzyme called Nagalase that prevents production of your GcMAF: that stops its 11 beneficial effects, and neutralises your immune system. So diseases become chronic, and cancer cells grow unchecked.

Minutes after a receiving a dose, 10 of the body's actions restart. In three weeks of two GcMAF 0.25ml doses a week, your immune system is rebuilt to above normal strength. You need two doses a week for typically 24 weeks for many diseases and early cancers, up to seven one ml doses a week and a year for stage 4 cancers. Your body then takes the disease down without side effects, and successfully in 80% of cases -depending upon how well you follow the protocol under "Treatment Protocol" on this website.

What is GcMAF?It is a human protein. One week's GcMAF looks like a small raindrop. If properly produced it is perfectly sterile, and a most ethical course for doctors.

GcMAF is therefore a replacement therapy for those who can't make their own. Taking GcMAF replaces the missing part of the immune system, and also acts as the body's own internal medicine.

GcMAF is extracted and isolated; its a 24 step process, and at the end it must have tests to prove its sterility and activity. (If it does not come with published tests, its probably not GcMAF.) One GcMAF has been tested in universities, laboratories and clinics, where, as a result of the testing, consistent activity and sterility have always been found, and been the subject of 40 scientific research papers.

What does GcMAF do?The GcMAF Conference 2013 showed GcMAF is a far more powerful molecule than thought, both in terms of the science, and doctors' results. In stage 4 cancer, some doctors who use the full protocol, listed on "Treatment Strategies," are saving every patient (if they have not had chemotherapy.) Success can be achieved with all tumour cancers including breast, lung, prostate, pancreatic and melanoma.

GcMAF can eradicate chronic inflammation and viral infections. It is better than antibiotics in many areas, and 25% successful with Autism, 50% or more with Chronic Herpes, Chronic Acne, Chronic cirrhosis of the liver, Chronic kidney disease, Chronic depression, Colitis, Crohn's, Fibromyalgia, Hepatitis, Herpes, LMBBS, ME/CFS, Osteoporosis, Periodontal disease, Psoriasis and various types of Immune dysfunction including allergies. Research shows GcMAF can halt deterioration in Parkinsons, multiple sclerosis (MS), dementia and ALS, and in its role of immune system regulator, can reverse diseases that attack the immune system like Lupus and Arthritis. And is effective with wound healing. Its successful with tumour cancers, and some others.

It abolishes neuropathic pain due to neuro-oxidative stress (stress due to the anti-cancer drug oxaliplatin) in the lab. (neurodegenerative diseases and autism that have oxidative stress as a pathogenetic mechanism)It increases neuronal connectivity by promoting differentiation and the formation of dendrites and neuritis (autism and ME/CFS, where there is a lack of connectivity between neurons).

See the 31 research papers published, particularly Brescia, and the 60 published by others listed under "The science".

80% of terminal stage four tumour cancers cases can be saved (40% if they've had chemo), but usually when they are closely monitored, which is why residential Treatment Centres are being run in Switzerland. If they have three months to live and have not had chemo, almost no one needs to be lost.

The 180 scientists who have published papers on trials of GcMAF selected those in the early stages of cancer and HIV, and reported nearly 100 percent success, with no recurrence after many years. They did not attempt trials on people with large tumours.

Our trials are quite different: many people are over 50, some over 80, with advanced or terminal cancers, with significant tumour mass. Most come to us when their doctors tell them they can do no more.

The life of GcMAF is only six days – you have to keep taking it until your disease has gone (ie your nagalase is under 0.65 nmol/min/mg) then a further 8 weeks, or the immune system gets shut down again.

How long should you take GcMAF for?8 weeks for chronic herpes/acne, fibromyalgia, inflammation.Allow 24 weeks plus of GcMAF for: Autism (85% improve, 25% eradication), CFS (70% eradication), HIV, Lyme (8% respond, most appear to have the VDR gene blocked and the viruses conceal themselves with biofilms) and stage 1 to 2 cancer, (80% respond).Late stage cancer, if you follow "Treatment Protocol" again has 80% responders, but it takes a year to 18 months to become cancer free.Cirrhosis of the liver: 16 months

Remember everyone responds differently. We can't say how you will respond.

The more minor the disease, the easier it is for GcMAF to eradicate. GcMAF needs normal levels of vitamin D to function strongly (take 10,000iu a day). in low responders, larger doses are required.

We have probably proved GcMAF can work for people up to age 90, and can destroy large tumour mass. See "Participants experiences".

If you have your blood taken for monocyte counts, relevant markers and vitamin D levels, and again for a nagalase test at the beginning, you should see on your next test after three weeks that your immune system is back to full strength, and after 8 weeks significantly falling nagalase will indicate the disease is losing its grip. Don't stop the GcMAF until your nagalase gets below 0.65 nmol/min/mg, when it loses the ability to prevent your body producing your own GcMAF, and then you no longer need ours. Even better, get scans.

Autism children can improve at five weeks with substantial improvements at 8 weeks. See "Participants experiences." But everyone is different.

The beauty of using your own immune system to attack disease or cancer is that it remembers how to defeat it for the rest of your life: it doesn't come back. And unlike chemotherapy, the side effects are trivial.

The only way you can tell if GcMAF is genuine and active is to test with living cells in a laboratory. See "Quality and Tests of our GcMAF." To recap:

We put live macrophages cells and MCF7 breast cancer cells together; nothing happens. Then we add GcMAF; in 72 hours the macrophages eat all the MCF7 cancer cells. We then put only GcMAF and MCF7 together, and the GcMAF turns the cancer cells back into healthy cells.

We have GcMAF available for preclinical trials. See "Buy GcMAF".

You must read at least all of "Buy GcMAF" and "Treatment strategies" on the left if you want to take this further. And you must be prepared to give us feedback.

Patent document on GcMAF

Cancerous cells and HIV-infected cells secrete -N-acetylgalactosaminidase into the blood stream, resulting in deglycosylation of serum Gc protein. This inactivates the MAF precursor activity of Gc protein, leading to immunosuppression... When peripheral blood monocytes/macrophages of 175 cancer patients bearing various types of cancer were treated in vitro with 100 pg GcMAF/ml, monocytes/macrophages (phagocytes) of all cancer patients were activated for phagocytic and superoxide generating capacity. This observation indicates that patient phagocytes are capable of being activated...

first heard about GcMAF almost a year ago. At the same time, I had first learned about "nagalase", a blood test that is used to in part determine whether or not one might be a candidate for GcMAF therapy. Nagalase is an enzyme that prevents Vitamin D receptors (VDR) from being activated on the surface of the macrophage. As a result, macrophages are not "activated" and our immune systems are not able to properly respond to invaders.

Here are some points that I have learned thus far on GcMAF:

- GcMAF has reportedly been tested more for safety, purity, etc. than other human blood products.- Macrophages are cultured, destroyed, and the GcMAF receptors are purified.- Treatment is via injection 1x/week for 8-20 weeks. Dose is titrated initially to avoid exacerbation or Herx responses as much as possible.- A commonly used dose is .25ml once weekly (a 2.2 ml vial should last 8 injections).- The primary test used in looking at whether or not GcMAF may be a reasonable intervention is nagalase.- Nagalase inactivates macrophages.- I personally would NEVER consider this option without having a baseline nagalase test. Normal is < 0.95. Mine was 2.9.

The practitioner I worked with suggested that 2.9 was in the range of someone with HIV or cancer in terms of the impact on the immune system. I'd like to hear from others in the Lyme community as you get test results as well to see if there is a pattern of elevated nagalase in those with Lyme disease. Whether or not Lyme itself has anything to do with nagalase elevation is something I have not been able to find anything on. We certainly all have underlying viral co-factors that are likely in play as well, but I suspect that Borrelia may also play a role in nagalase elevation.

- In healthy college students, a nagalase 0.4 is not uncommon (the lower the better).

- At 2.9, my practitioner was surprised that I did not have more cognitive deficits such as memory loss and other cognitive issues.

- It has been suggested that ongoing antimicrobial therapy without a working immune system is like leaving the house with the door wide open inviting burglars in. By using GcMAF to activate macrophages, nagalase drops, and one may regain a functional immune system. The door is then closed to further invaders and we may no longer serve as a microbe hotel.

- Maintenance therapy should not be needed once the immune system is once again properly functioning.

- Activated macrophages only remain active for 7 days so any negative responses are generally short-lived. That said, some people do have strong inflammatory responses that are not believed to be typical die-off reactions.

- It has been indicated that in some cases, other medications may be needed in order to manage the inflammatory response. This is another reason that one needs to be working closely with a knowledgeable practitioner before considering GcMAF in my opinion. In the CFS and GcMAF world, this more severe form of a die-off reaction is called IRIS.

- VDR genetics do not seem to play a role in predicting response as earlier thought according to one practitioner that I have spoken with. That said, Vitamin D levels do correlate with the positive response rate of GcMAF. Thus, Vitamin D supplementation may be required in order to optimize outcome.

- Other than die-off reactions or activation of symptoms (inflammation), no other side effects are generally expected.

- Nagalase should be monitored every 1-2 months while on treatment to determine the required duration of the therapy. Target nagalase after treatment would be 0.4 to 0.6.

- Elevated nagalase has a profound detrimental effect on the immune system. Elevated nagalase is often presumed to be related to microbes of viral origin or cancer. Viruses that are nagalase producers open the door to chronic infections.

- Hemagglutinin contains nagalase and is also found in flagella of some bacteria so it could also be the case that some bacteria may produce nagalase.

- Parents with ASD children also often have elevated nagalase.

- A practitioner I spoke with likened Lyme disease to a "peat moss fire" burning below the surface. Activating macrophages should help to deal with the fire.

- GcMAF should be helpful in dealing with other infections that are not of viral origin; for example, Borrelia, Bartonella, and other infections commonly associated with Tick-Borne Infections (TBIs). GcMAF is active against many cancers and many different kinds of microbes.

- Neopterin is another test that is sometimes used as an indicator of immune suppression. As macrophages become activated, neopterin may rise and later fall. If one is in the normal range for neopterin and has an immune-related illness, this could be an indication that the immune system is suppressed and not responding appropriately.

- People with autoimmune conditions can generally use GcMAF. However, GcMAF may be contraindicated in people with Multiple Sclerosis.

- Reduction in nagalase is generally seen early in the course of treatment; within the first 3-6 weeks. In some studies, nagalase dropped by over 50% in less than six weeks.

- Cancer patients may initially feel as bad on GcMAF as they do on chemotherapy, but often feel much better after the first month.

- Anti-inflammatories may limited the effect of GcMAF.

- Enzymes and biofilm-reducing supplements may have a negative impact on GcMAF therapy and may be best avoided. It is still too early to know what the impact may be, but one practitioner I spoke with feels that it is best to avoid these.

- One should not be on any immune-suppressing agents while on GcMAF as the immune system must be partially functional in order to respond appropriately to the treatment.

- A common pattern is to see elevated lymphocytes, high nagalase, and low NK cells. Once nagalase drops, it may be the case that NK cell function could be positively impacted. CD57 is a type of NK cell. It is too early to know if this proves to be true, but it is one of the things I'm quite interested in.

Researchers testing GcMAF stated it, "works 100% of the time to eradicate cancer completely, and cancer does not recur even years later." (This was stated based on the tested group of patients -nothing works 100% for everyone) The weekly injection GcMAF, a harmless glyco-protein activates the human immune system which then can kill the growing cancer. Studies among breast cancer and colon cancer patients produced complete remissions lasting 4 and 7 years respectively. This glyco-protein 'cure' is totally without side effect but currently goes unused and completely ignored by cancer doctors. Why? Maybe it is because there is little money to be made in selling it. For less than $2000USD a cancer patient can obtain an adequate amount of GcMAC.

When human macrophages were treated in vitro with 100 pg GcMAF/ml for 3 hours and a prostate cancer cell line LNCaP was added with an effector/target ratio of 1.5, approximately 51% and 82% of LNCaP cells were killed by 4 and 18 hours of incubation, respectively [14,15]. This in vitro tumoricidal capacity of macrophages activated by GcMAF led us to investigate the therapeutic efficacy of GcMAF for prostate cancer. GcMAF therapy as a single remedy modality can eradicate metastatic breast and colorectal cancers most effectively...